Viral Hepatitis
Copyright ©The Author(s) 2002. Published by Baishideng Publishing Group Inc. All rights reserved.
World J Gastroenterol. Oct 15, 2002; 8(5): 868-871
Published online Oct 15, 2002. doi: 10.3748/wjg.v8.i5.868
Lamivudine does not increase the efficacy of interferon in the treatment of mutant type chronic viral heaptitis B
Sien-Sing Yang, Chao-Tien Hsu, Jui-Ting Hu, Yung-Chih Lai, Chi-Hwa Wu
Sien-Sing Yang, Jui-Ting Hu, Yung-Chih Lai, Chi-Hwa Wu, Liver Unit, Cathay General Hospital, Taipei, Taiwan, China
Sien-Sing Yang, Chao-Tien Hsu, Medical Faculty, China Medical College and Hospital, Taichung, Taiwan, China
Author contributions: All authors contributed equally to the work.
Correspondence to: Sien-Sing Yang, MD, Liver Unit, Cathay General Hospital, 280 Sec. 4, Jen-Ai Rd., Taipei, Taiwan 10650. yangss@seed.net.tw
Telephone: +886-2-2708-2121 Ext.3121 Fax: +886-2-2707-4949
Received: April 12, 2002
Revised: June 1, 2002
Accepted: June 11, 2002
Published online: October 15, 2002
Abstract

AIM: To study the role of lamivudine in improving the efficiency of interferon for the treatment of mutant type chronic hepatitis B.

METHODS: Fifteen patients with mutant type chronic hepatitis B were prospectively studied. All patients had liver histology and serology to prove the diagnosis of chronic hepatitis B. Each patient received 4.5 millionunits of interferon alpha-2a thrice weekly and 100 mg of oral lamivudine daily for 24 wk. Patients were observed and tested for blood chemistry every week for the initial 4 wk and every 2 wk thereafter during the treatment until 24 wk. After the end of treatment, patients were followed up at 4-week intervals for an additional 6 mo. Serum HBV DNA levels were tested using the liquid phase molecular hybridization assay. Those with non-detectable HBV DNA were also tested using the real-time polymerase chain reaction. One patient, who did not finish treatment due to depression, was excluded.

RESULTS: At the end of treatment, 7 (50%) patients had serum ALT levels within normal limits; 12 (86%) patients had serum HBV DNA levels < 5 pg/mL using the liquid phase molecular hybridization assay, but only 8 (67%) were < 20 copies/dL using the real-time polymerase chain reaction. Six months after treatment, only two (14%) patients had a sustained complete response to the combination therapy with serum ALT level < 35 iu/L and undetectable serum HBV DNA levels.

CONCLUSION: These pilot data showed that lamivudine did not increase the efficacy of interferon in the treatment of mutant type chronic hepatitis B. The liquid phase molecular hybridization assay was not sensitive enough to detect the low HBV DNA levels during combined interferon and lamivudine therapy.

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